Tekin Mustafa, Akcayoz Duygu, Incesulu Armagan
Division of Pediatric Molecular Genetics, Ankara University School of Medicine, Ankara, Turkey.
Am J Med Genet A. 2005 Sep 15;138(1):6-10. doi: 10.1002/ajmg.a.30907.
Screening of 12 Turkish families with apparently autosomal recessive nonsyndromic sensorineural deafness without GJB2 and mtDNA m.1555A > G mutations for 11 previously mapped recessive deafness loci showed a family in which hearing loss cosegregated with the DFNB9 (OTOF) locus. Three affected children were later found to carry a novel homozygous c.3032T > C (p.Leu1011Pro) mutation in the OTOF gene. Both parents were heterozygous for the mutation. p.Leu1011Pro alters a conserved leucine residue in the C2D domain of otoferlin. Pure tone audiometry of the family showed severe to profound sensorineural hearing loss (with U-shape audiograms) in children, and normal hearing in the parents. Otoacoustic emissions and auditory brainstem response (ABR) suggested the presence of auditory neuropathy in affected individuals.
对12个患有明显常染色体隐性非综合征性感音神经性耳聋且无GJB2和线粒体DNA m.1555A>G突变的土耳其家庭,针对11个先前定位的隐性耳聋基因座进行筛查,结果发现一个家庭中听力损失与DFNB9(OTOF)基因座共分离。后来发现三个患病儿童在OTOF基因中携带一种新的纯合c.3032T>C(p.Leu1011Pro)突变。父母双方均为该突变的杂合子。p.Leu1011Pro改变了otoferlin的C2D结构域中一个保守的亮氨酸残基。该家庭的纯音听力测试显示,儿童存在重度至极重度感音神经性听力损失(听力图呈U形),而父母听力正常。耳声发射和听觉脑干反应(ABR)提示患病个体存在听觉神经病。
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